Site selection in global clinical trials in patients hospitalized for heart failure: perceived problems and potential solutions

被引:0
|
作者
Mihai Gheorghiade
Muthiah Vaduganathan
Stephen J. Greene
Robert J. Mentz
Kirkwood F. Adams
Stefan D. Anker
Malcolm Arnold
Fabio Baschiera
John G. F. Cleland
Gadi Cotter
Gregg C. Fonarow
Christopher Giordano
Marco Metra
Frank Misselwitz
Eva Mühlhofer
Savina Nodari
W. Frank Peacock
Burkert M. Pieske
Hani N. Sabbah
Naoki Sato
Monica R. Shah
Norman L. Stockbridge
John R. Teerlink
Dirk J. van Veldhuisen
Andrew Zalewski
Faiez Zannad
Javed Butler
机构
[1] Northwestern University Feinberg School of Medicine,Center for Cardiovascular Innovation
[2] Harvard Medical School,Department of Medicine, Massachusetts General Hospital
[3] Duke University Medical Center,Division of Cardiology, Department of Medicine
[4] University of North Carolina School of Medicine,Division of Cardiology
[5] Centre for Clinical and Basic Research,Castle Hill Hospital
[6] University of Western Ontario,Division of Cardiology
[7] Novartis Pharma AG,Division of Cardiology
[8] Hull York Medical School,Department of Emergency Medicine
[9] Momentum-Research,Division of Cardiology
[10] Inc.,Department of Medicine
[11] University of California,Department of Internal Medicine and Cardiology
[12] Quintiles,Center for Drug Evaluation and Research
[13] Cardiovascular and Metabolic Therapeutic Delivery Unit,Section of Cardiology, San Francisco Veterans Affairs Medical Center
[14] University of Brescia,Department of Cardiology
[15] Bayer Healthcare Pharmaceuticals,Inserm CIC 9501 and U961
[16] Bayer Vital GmbH,Division of Cardiology
[17] Baylor College of Medicine,undefined
[18] Medical University of Graz,undefined
[19] Henry Ford Hospital,undefined
[20] Nippon Medical School Musashi-Kosugi Hospital,undefined
[21] National Heart Lung and Blood Institute,undefined
[22] US Food and Drug Administration,undefined
[23] University of California,undefined
[24] University of Groningen,undefined
[25] Novartis Pharmaceutical Corporation,undefined
[26] Université de Lorraine,undefined
[27] CHU Cardiology,undefined
[28] Emory University School of Medicine,undefined
来源
Heart Failure Reviews | 2014年 / 19卷
关键词
Heart failure; Site selection; Clinical trials; FDA;
D O I
暂无
中图分类号
学科分类号
摘要
There are over 1 million hospitalizations for heart failure (HF) annually in the United States alone, and a similar number has been reported in Europe. Recent clinical trials investigating novel therapies in patients with hospitalized HF (HHF) have been negative, and the post-discharge event rate remains unacceptably high. The lack of success with HHF trials stem from problems with understanding the study drug, matching the drug to the appropriate HF subgroup, and study execution. Related to the concept of study execution is the importance of including appropriate study sites in HHF trials. Often overlooked issues include consideration of the geographic region and the number of patients enrolled at each study center. Marked differences in baseline patient co-morbidities, serum biomarkers, treatment utilization and outcomes have been demonstrated across geographic regions. Furthermore, patients from sites with low recruitment may have worse outcomes compared to sites with higher enrollment patterns. Consequently, sites with poor trial enrollment may influence key patient end points and likely do not justify the costs of site training and maintenance. Accordingly, there is an unmet need to develop strategies to identify the right study sites that have acceptable patient quantity and quality. Potential approaches include, but are not limited to, establishing a pre-trial registry, developing site performance metrics, identifying a local regionally involved leader and bolstering recruitment incentives. This manuscript summarizes the roundtable discussion hosted by the Food and Drug Administration between members of academia, the National Institutes of Health, industry partners, contract research organizations and academic research organizations on the importance of selecting optimal sites for successful trials in HHF.
引用
收藏
页码:135 / 152
页数:17
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